An Interview with Dr. Sanjay Kaul

The FDA Advisory Committee member reveals what lies ahead for Invokana and SGLT-2 inhibitors

Dr. Sanjay Kaul is a noted cardiologist working at the Cedars-Sinai Medical Center in Los Angeles. For the past several years, he has served as a cardiology expert on the FDA's Endocrine and Metabolic Advisory Committee (EMDAC), meaning he is part of the team that evaluates all new diabetes drugs up for FDA approval, with a particular eye toward the drugs' cardiovascular risks. In this role, he has unquestionably become one of the most influential panel members – his astute comments have not only affected the views of fellow panel members, but arguably those of the FDA when it makes its final decisions on drug approval.

Earlier this month, Dr. Kaul was part of the 15-member panel that reviewed J&J's Invokana (canagliflozin), which appears on track to be the first SGLT-2 inhibitor approved in the United States. Dr. Kaul was one of ten votes in favor of the drug, and his recommendation came with a critical caveat (and one that we assume all the panelists would have agreed on): Invokana should be used only by those with normal or mildly impaired kidney function, as the drug will be most optimally used (both in terms of efficacy and safety) in patients who do not have any serious kidney problems. After the conclusion of the advisory panel meeting, we had an opportunity to speak with Dr. Kaul, who was very generous with his time. He shared some critical insights with us, including his thoughts on the 10-5 vote for approval, why SGLT-2 inhibitors might have more major potential for people with type 1 diabetes, and why the FDA is unlikely to approve any use of Invokana by people with moderate to severe renal impairment.

Dr. Kaul on what the advisory panel's 10-5 vote in favor of approval means for the FDA and going forward:

If canagliflozin's FDA Advisory Committee panel is not a strong argument for doing away with the voting, then I don't know what will. The inverse relationship between the vote and the discussion was quite hilarious. Only the media and the analysts are interested in the vote count. No one should interpret the 10-5 vote as a strong endorsement for canagliflozin, in my opinion. I think I made it clear that my "yes" vote came with the caveat that the sponsor had shown benefit exceeding risk only in patients with normal or mildly impaired renal function. Despite the fact that the sponsor followed the protocol approved by the FDA, I have significant concerns with the CV safety assessment program. However, the sponsor (J&J) should not be penalized for this. The FDA has to provide increased clarity regarding the issues raised by the canagliflozin new drug application (NDA).

Dr. Kaul on prospects for SGLT-2 inhibitors as part of a treatment program for people with type 1 diabetes:

Type 1 diabetes might be a more desirable population for canagliflozin given the limited therapeutic choices and unique mechanism of action with no weight gain or hypoglycemia liability. Some other Advisory Committee members also felt that the drug might be better positioned for type 1 patients without obvious moderate to severe renal dysfunction.

Dr. Kaul on safety questions associated with SGLT-2 inhibitors, starting with whether SGLT-2 inhibitors can be used by people with moderate renal impairment:

That is unlikely to pass the FDA's muster, as the benefit-risk balance is not desirable for such patients. I was surprised that J&J did not rigorously address the kidney disease concerns (the company did not collect detailed data on these events). If more than 50% of patients enrolled in the trial have moderatly impaired kidney function, then this therapy is unlikely to be of value in these high-risk patients even if unacceptable cardiovascular safety is ruled out. The SCOUT (use of the drug sibutramine for obesity) dilemma is revisited here – one is forced to evaluate cardiovascular safety in a population that is unlikely to be a target for therapy!

An interesting concept, but the long-term safety of SGLT-2 inhibitors with regards to infections (and potential risk of cancer) remains incompletely characterized. This strategy has been successfully implemented with Janumet (Januvia plus metformin), so there is reason to be optimistic.

Thank you so much to Dr. Kaul for spending time with diaTribe and sharing his views with us. We thank him on behalf of patients for contributing so much time to this important government advisory board.

This article is published on dLife thanks to diaTribe (www.diaTribe.us), an independent, advertising-free e-newsletter for everyone eager to learn about the latest advances in diabetes management. diaTribe is your inside track on diabetes research and products — sign up here for your complimentary lifetime subscription!

NOTE: This information is not intended to be a replacement or substitute for consultation with a qualified medical professional or for professional advice related to diabetes or another medical condition. Please contact your physician or medical professional with any questions and concerns about your medical condition.

Last Modified Date: June 24, 2013

All content on dLife.com is created and reviewed in compliance with our editorial policy.

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